肠道菌群在调节内皮生长分化、保护细胞以及维持免疫稳态等方面具有比较重要的作用。近几年的研究报道，肠道菌群失调可能会导致多种骨关节疾病的发生。肠道菌群失调而引起机体产生炎症反应等可能参与了类风湿关节炎的发病机制，临床口服莫西沙星和低淀粉饮食可以减轻类风湿关节的症状，此外乳酸菌类制剂在临床治疗类风湿关节炎方面也具有良好的效果。从而在临床上可以通过靶向调节肠道菌群失调而治疗类风湿关节炎患者，提供了理论新方向。

[1] QIN J,LI R,RASE J,et al.A human gut microbialgene catalogue established by metagenomic sequencing[J].Nature,2010,464(7285):59-65.
[2] KHAMMA S,TOSH P K.Aclinician's primer on human health and disease[J].Mayo Clin Proc,2014,89(1):107-114.
[3] 杨泽冉,辛毅,侯洁,等.肠道菌群失调及其相关疾病研究进展[J].山东医药,2016,56(1):99-101.
[4] CROSS M,SMITH E,HOY D,et al.The global burden of rheumatoid arthritis:estimates from the global burden of disease 2010 studuy[J].Ann Rheum Dis,2014,73(7):1316-1322.
[5] TOIVANEN P.Normal intestinal microbiota in the aetiophthogenesis of rheumatoid arthritis[J].Ann Rheum Dis,2003,62(9):807-811.
[6] ZHANG X,ZHANG D,JIA H,et al.The oraland gut microbimomes are perturbed in rheumatoid arthritis and partly normalized after treament[J].Nat Med,2015,21(8):895-905.
[7] PASZTOI M,MISIAK P,GYORGY B,et al.Infection and autoimmunity:Lessons of animal models[J].Eur J Microbiol Immunol(Bp),2011,1(3):198-207.
[8] AUGER I,ROUDIER J.A function for the QKRAA amino acid motif:mediating binding of DnaJ to DnaK.Implications for the association of rheumatoid arthritis with HLA-DR4[J].J Clin Invest,1997,99(8):1818-1822.
[9] WU H J,IVANOV.Ⅱ,DARCE J,et al.Gut residing segmented filamentous bacteria drive autoimmune arthritis via T helper 17cells[J].Immunity,2010,32(6):815-827.
[10] YOSHITOMI H,SAKAGUCHI N,KOBAYASHI K,et al.A role for fungal(beta) ghcans and their receptor Dectin-1 in the induction of autoimmune arthritis in genetically susceptible mice[J].J Exp Med,2005,201(6):949-960.
[11] KIM D,YOO S A,KIM W U.Gut microbiota in autoimmunity:potential for clinical applications[J].Arch Pharm Res,2016,39(11):1565-1576.
[12] TURNBAUGH P J,LEY R E,HAMADY M,et al.The human micro-biome project[J].Nature,2007,449(7164):804-810.
[13] SCHROEDER B O,BACKHED F.Signals from the gut microbiota to distant organs in physiology and disease[J].Nat Med,2016,22(10):1079-1089.
[14] ROSENBAUM J T,ASQUITH M J.The mierobiome:A revolution in treatment for rheumatic diseases?[J].Curr Rheumatol Rep,2016,18(10):62-62.
[15] DUBILIER N,MCFALL-NGAI M,ZHAO L.Microbiology:Create a global microbiome effort[J].Nature,2015,526(7575):631-634.
[16] ZAISS M M,RAPIN A,LEBON L,et al.The intestinal microbiota contributes to the ability of helminths to modulate allergic inflammation[J].Immunity,2015,43(5):998-1010.
[17] SIVAN A,CORRALES L,HUBERT N,et al.Commensal bifidobaete-rium promotes antitumor immunity and facilitates anti-PD-L1 effieacy[J].Science,2015,350(6264):1084-1089.
[18] VETIZOU M,PITT J M,DAILLERE R,et al.Antieancer immunotber-apy by CTLA-4 blockade relies on the gut mierobiota[J].Seience,2015,350(6264):1079-1084.
[19] VIJAY-KUMAR M,AITKEN J D,CARVALHO F A,et al.Metabolic syndrome and altered gut mierobiota in mice lacking Toll-like receptor 5[J].Science,2010,328(5975):228-231.
[20] LEY R E,BAEKHED F,TURNBAUGH P,et al.Obesity alters gut microbial ecology[J].Proe Natl Acad Sci U S A,2005,102(31):11070-11075.
[21] MANICHANH C,BORRUEL N,CASELLAS F,et al.The gut microbiota in IBD[J].Nat Rev Gastroenterol Hepatol,2012,9(10):599-608.
[22] OCHOA-REPARAZ J,MIELCARZ D W,WANG Y,et al.A polysaccha-ride from the human commensal Bacteroides fragilis protects against CNS demyelinating disease[J].Mucosal Immunol,2010,3(5):487-495.
[23] DE ANGELIS M,FRANCAVILLA R,PICCOLO M,et al.Autism spectrum disorders and intestinal microbiota[J].Gut Microbes,2015,6(3):207-213.
[24] VAN PRAET J T,DONOVAN E,VANASSCHE I,et al.Commensal microbiota influence systemic autoinlmune responses[J].EMBO J,2015,34(4):466-474.
[25] COSTELLO M E,CICCIA F,WILLNER D,et al.Brief Report:Intestinal Dysbiosis in Ankylosing Spondylitis[J].Arthritis Rheumatol,2015,67(3):686-691.
[26] WU H J,WU E.The role of gut microbiota in immune homeostasis andautoimmunity[J].Gut Microbes,2012,3(1):4-14.
[27] LIU X,ZOU Q,ZENG B,et al.Analysis of fecal lactobacillus community structure in patients with early rheumatoid arthritis[J].Curr Microbiol,2013,67(2):170-176.
[28] VAAHTOVUO J,MUNUKKA E,KORKEAMÄKI M,et al.Fecal microbiota in early rheumatoid arthritis[J].J Rheumatol,2008,35(8):1500-1505.
[29] VAGHEFMEHRABANY E,ALIPOUR B,HOMAYOUNIRAD A,et al.Probiotic supplementation improves inflammatory status in patients with rheumatoid arthritis[J].Nutrition,2014,30(4):430-435.
[30] 庞立园,丁锐,张瑾,等.两歧双歧杆菌对菌群失衡大鼠类风湿关节炎的调整作用[J].中国微生态学杂志,2016,28(9):999-1001.
[31] SCHER J U,SCZESNAK A,LONGMAN R S,et al.Expansion of intestinal Prevotella copri correlates with enhanced susceptibility to arthritis[J].Elife,2013,2(1629):e01202.
[32] MAEDA Y,KURAKAWA T,UMEMOTO E,et al.Dysbiosis contributes to arthritis development via activation of autoreactive T cells in the intestine[J].Arthritis Rheum,2016,68(11):2646-2661.
[33] ZHANG X,ZHANG D,JIA H,et al.The oral and gut microbiomes are perturbed in rheumatoid arthritis and partly normalized after treatment[J].Nat Med,2015,21(8):895-905.
[34] LUCKHEERAM R V,ZHOH R,VERMA A D,et al.CD4(+) T cells:differentiation and functions[J].Clin Dev Immunol,2012,2012(12):925135-925135.
[35] HARRINGTON I,E,HATTON R D,MANGAN P R,et al.Interleukin 17 producing CD4⁺ effector T cells develop via a lineage distinct from the T helper type l and 2 lineages[J].Nat Immuno,2005,6(11):1123-1132.
[36] WEAVER C T,HARRINGTON L E,MANGANP R,et al.Th17:An effector CD4 T cell lineage with regulatory T cell ties[J].Immunity,2006,24(6):677-688.
[37] MIYARA M,ITO Y,SAKAGUCHI S.TREG-ceil therapies for autoimmune rheumatic diseases[J].Nat Rev Rheumatol,2014,10(9):543-551.
[38] SMITH K,MCCOY K D,MACPHERSON A J.Use of axenic animals in studying the adaptation of mammals to their commensal intestinal microbiota[J].Semin Immunol,2007,19(2):59-69.
[39] IVANOV I I,ATARASHI K,MARIEL N,et al.Induction of intestinal Th17 cells by segmented filamentous bacteria[J].Cell,2009,139(3):485-498.
[40] ROUND J L,LEE S M,LI J,et al.The Toll like receptor 2 path-way establishes colonization by a commensal of the human microbiota[J].Seience,2011,332(6032):974-977.